DE102014115951A1 - Compositions containing finafloxacin and tris - Google Patents

Abstract

Finafloxacin was found to have high solubility in the presence of tris. This solubility is significantly higher than in the presence of other substances commonly used as buffers (e.g., phosphate buffers). The observed significant increase in the solubility of finafloxacin in compositions containing Tris additionally advantageously accompanies the long-term stability of such solutions. Tris is thus considered a specific agent, which significantly increases the solubility of finafloxacin in solutions. By preparing compositions comprising Tris, it is possible to stably dissolve finafloxacin in such an amount that these compositions can be effectively used as parenteral compositions for the treatment of bacterial infections.

Description

Background of the invention

The present invention relates to compositions containing finafloxacin and tris. Such compositions may be pharmaceutically acceptable parenteral compositions and used to treat bacterial infections such as urinary tract infections, intra-abdominal infections, skin and soft tissue infections, diabetic foot infections, bacteremia and respiratory infections.

Finafloxacin (International Non Proprietary Name) is an antibiotic of the class of quinolonecarboxylic acids of the formula: 8-cyano-1-cyclopropyl-6-fluoro-7 - ((1S, 6S) -2-oxa-5 , 8-diazabicyclo [4.3.0] non-8-yl) -1,4-dihydro-4-oxo-3-quinolinecarboxylic acid. Finafloxacin and derivatives thereof can be obtained by in the WO 98/26779 Matzke et al., the contents of which are incorporated herein by reference in their entirety. Finafloxacin has been shown to be useful in the treatment of H. pylori infections ( EP0946176 ), eye, ear or nose infections ( US 8,536,167 ).

WO 98/26779 . EP 0946176 or US 8,536,167 however, do not describe pharmaceutical formulations suitable for parenteral administration. Parenteral administration of drugs is particularly important for the treatment of ICU patients who are often unable to take oral medications. In addition, parenteral administration may also help to rapidly reduce the number of pathogens at an infection site due to the rapid release of the drug into the bloodstream.

For parenteral use, finafloxacin must be formulated as a stable, effective composition containing a pharmaceutically sufficient amount of the active ingredient in an acceptable small volume. This means that relatively high levels of finafloxacin must be reliably and stably dissolved. In order to store the pharmaceutical formulation over a longer period of time, a disintegration of the pharmaceutical agent or an excipient must be avoided.

When using and handling finafloxacin, the solution properties are known to be a common problem. The solubility of finafloxacin is considered insufficient to produce physically stable solutions of sufficiently high concentration at acceptable pH levels so that infections can be treated with a physiological solution. The instability manifests itself by the formation of visible and non-visible particles during storage. In addition, because of the poor solubility of finafloxacin, there is the problem that a solution having a composition containing, for example, 200 mg to 1000 mg of the active ingredient or more can be administered parenterally in an acceptable volume.

Thus, there is a need for compositions containing adequate levels of finafloxacin in an acceptable volume and additionally having long-term stability properties so that they can be used as pharmaceutical compositions for parenteral applications.

Brief description of the invention

Surprisingly, it has been found that finafloxacin has a high solubility in the presence of tris. This solubility is significantly higher than in the presence of other substances that are typically used as buffers (e.g., phosphate buffers). The observed significant increase in the solubility of finafloxacin in compositions containing Tris additionally advantageously accompanies the long-term stability of such solutions. Both effects lead to a completely unexpected result. Tris can therefore be considered as a special means of significantly increasing the solubility of finafloxacin in solutions. By preparing compositions containing Tris, it is possible to stably dissolve finafloxacin in a sufficient amount so that these compositions can be effectively used as parenteral solutions for the treatment of bacterial infections. Suitable compositions according to the invention contain 1 to 6 g / l finafloxacin, 7 to 8 g / l NaCl, 1 to 2 g / l Tris at a pH of 8.0 to 8.5. A specific composition according to the invention is for example a composition containing 3.2 g / l finafloxacin, 7.8 g / l NaCl, 1.21 g / l Tris at a pH of 8.25.

Detailed description of the invention

The compositions of the present invention include finafloxacin and Tris. Tris is the abbreviation for 2-amino-2-hydroxymethyl-propane-1,3-diol or tris (hydroxymethyl) -aminomethane. Another abbreviation for Tris is THAM. The chemical formula is (HIGH ₂ ) ₃ CNH ₂ . Tris is known as one of the most commonly used buffers in biochemistry and molecular biology. The effective buffer range is between 7 and 9, which is the typical physiological pH range of most living organisms. A common form of Tris is Tris hydrochloride (Tris-HCl). In higher concentrations, Tris is used as an alternative to sodium bicarbonate as an anti-hyperacidity agent.

The term "tris" in the context of the compositions according to the invention is intended to include all chemical forms of Tris including, without limitation, the free base, the conjugated acid (Tris-HCl), all Tris salts and all derivatives of Tris, and all others Substances having the same or similar mechanism of action as Tris in the alkaline pH range, as specified and claimed in connection with the compositions according to the invention.

Comparisons with other buffers, for example phosphate, or with a pH-adjusted solution in water for injections (Wfl) showed that Tris significantly increases the solubility of finafloxacin. This result shows that, surprisingly, Tris itself has a remarkable solubilizing effect on finafloxacin. This effect is new and independent of Tris' ability to buffer a solution. Another advantage is that the use of Tris, due to its buffer capacity in the alkaline pH range, prevents a pH decrease during storage or when, for example, is diluted with isotonic sodium chloride (NaCl). A preferred composition according to the invention has a pH of 8.0 to 8.5.

The compositions according to the invention may contain Tris concentrations in the range from about 0.001 M to 0.2 M, preferably the concentration is from 0.002 M to 0.1 M. A suitable composition according to the invention has for example a Tris concentration of 0.01 M The use of approximately equimolar amounts of tris and finafloxacin in the compositions according to the invention is preferred.

Using tris within the above indicated concentrations and pH ranges as an ingredient in the compositions according to the invention, it is possible to prepare pharmaceutically acceptable parenteral compositions. Due to the improved solubility of finafloxacin in compositions containing Tris, finafloxacin concentrations suitable for pharmaceutical applications can be achieved. The term "pharmaceutically acceptable" is known to those skilled in the art and refers to compositions, polymers and other materials and / or dosage forms that are of reasonable value for risk according to the judgment of one skilled in the art for use in contact with human and human tissues Animals, without causing excessive toxicity, irritation, allergic reaction or other problems or complications.

Embodiments of the compositions of the present invention comprise one or more carriers or adjuvants. Excipients / adjuvants commonly used in pharmaceutical compositions include, but are not limited to, isotonizing agents, preservatives, chelating agents, buffers, surfactants, antioxidants and free-radical scavengers. Other adjuvants are solubilizers, stabilizers, comfort enhancing agents, polymers, plasticizers, pH adjusting agents and / or lubricants. In preferred embodiments according to the present invention, the concentrations of the excipients are typically 0.1 to 100 times the concentration of finafloxacin. The excipients are selected based on their inertness against finafloxacin. The amount of the excipients should be chosen so that preferably a tonicity of 200 to 700 mOsmol / kg, particularly preferably from 260 to 390 mOsmol / kg, is achieved. Examples of isotonizing agents include, but are not limited to, NaCl, glucose, fructose, maltose, sorbitol, sucrose, xylitol, glycerol (glycerol / glycine), mannitol, or mixtures thereof.

A preferred salt in the compositions according to the invention is sodium chloride. NaCl concentrations of 0.4% to 1.0% (w / v) are suitable, a range from 0.6% to 0.9% (w / v) of sodium chloride is preferred, and a concentration of 0.7% to 0.8% is particularly preferred ( w / v) sodium chloride. Generally, a range of 260 to 390 mOsmol / kg is considered to be isotonic. Compositions according to the invention may contain 7.8 g / l NaCl to obtain 280 mOsmol / kg.

The term "finafloxacin" in the context of the compositions of the present invention is intended to include finafloxacin HCL, finafloxacin free base and other pharmaceutically acceptable salts, enantiomers or hydrates. Diastereomer and enantiomerically pure finafloxacin is preferred for use in the embodiments of the present invention.

A preferred salt in certain embodiments of the present invention is finafloxacin monohydrochloride. However, common pharmaceutically acceptable salts of finafloxacin may also be used, including, but not limited to, salts with pharmaceutically acceptable, inorganic and organic acids such as acetic, lactic, succinic, maleic, malic, tartaric, citric, gluconic, ascorbic, benzoic, Naphthalene-1,5-disulfonic acid, naphthalene-2-sulfonic acid, cinnamic acid, fumaric acid, dihydroxyfumaric acid, glutamic acid, oxaloacetic acid, glutaric acid, salicylic acid, phosphoric acid, hydrochloric acid, hydrobromic acid, hydroiodic acid, sulfamic acid, pivalic acid, stearic acid, 1,2-ethanedisulfonic acid, isethionic acid, sulfuric acid , Methanesulfonic acid, ethanesulfonic acid, benzenesulfonic acid, toluenesulfonic acid, sulfonic acids and the like. Also suitable as salts are those of inorganic or organic bases, such as KOH, NaOH, Ca (OH) ₂ , Al (OH) ₃ , piperidine, morpholine, ethylamine, triethylamine, arginine and the like. Included within the scope of the invention are the hydrogenated forms of the compounds containing various amounts of water or as solvates with other solvents. Non-limiting examples of hydrates include monohydrates, dihydrates, etc. Non-limiting examples of solvates include ethanol solvates, acetone solvates, etc.

Pharmaceutically customary compositions according to the invention comprise finafloxacin in a concentration of 0.2 g / l to 50 g / l, preferably in a concentration of 0.4 g / l to 25 g / l, particularly preferably in a concentration of 0.8 g / l to 13 g / l. Preferred embodiments of the invention are compositions comprising 1 to 6 g / L finafloxacin, 7 to 8 g / L NaCl and 1.0 to 2 g / L Tris. A specific composition according to the invention is for example a composition containing 3.2 g / l finafloxacin, 7.8 g / l NaCl and 1.21 g / l Tris. Such compositions preferably have a pH of about 8.0 to 8.5 and especially a pH of 8.25.

In particular embodiments, the compositions of the present invention are administered once daily. However, the compositions of the present invention may also be formulated for administration in any other frequency of administration, including twice daily, three times a day, every two days, or a greater or lesser frequency, at regular or irregular intervals, that change or remain constant. Such a dosing frequency is also maintained for a varying amount of time depending on the therapy regimen. The duration of a particular regimen may vary from once-daily dosing to a regimen that lasts for days, weeks, or months. One skilled in the art will be familiar with the determination of the regimen for a particular indication that includes a pharmaceutically effective amount of finafloxacin or a composition thereof. The term "pharmaceutically effective amount" is a known technical term and refers to the amount of an agent which, when incorporated into a pharmaceutical composition of the present invention, produces the desired effect at a reasonable benefit / risk ratio on any medical treatment , The effective amount may vary depending on such factors as the disease or infectious agent being treated, the particular composition administered, or the severity of the disease or pathogen.

The compositions of the invention are particularly useful for treating mammals and humans who have a microbial infection or who could get it with some risk. Certain embodiments of the present invention may also be preferably used prophylactically to prevent infection by an infectious agent. The compositions according to the invention can be used effectively for the treatment of bacterial infections such as urinary tract infections, abdominal infections, skin and soft tissue infections, diabetic foot infections, bacteremia, prostatitis, bone and joint infections, respiratory infections, etc.

The compositions according to the invention may be prepared by conventional methods for the preparation of aqueous pharmaceutical compositions known to those skilled in the art. The administration of embodiments of such compositions for the treatment of bacterial infections or for prophylactic use to prevent infection of mammals or humans can be accomplished by various methods known to one skilled in the art.

Examples

Example 1: Solubility of finafloxacin HCl

The solubility of finafloxacin in the form of the monohydrochloride salt was tested at pH's between 7.3 and 9.0 using the following solutions:
0.01 M Tris: water for injections 800 ml; 1.21 g Tris; Sodium chloride 7.5 g, water for injections ad 1000 ml; the pH was adjusted with HCl / NaOH.

0.025 M phosphate: water for injections 800 ml, sodium dihydrogen phosphate 1,950 g, disodium hydrogen phosphate 2,225 g, sodium chloride 7,5 g, water for injections ad 1000 ml; the pH was adjusted with HCl / NaOH.

WfI: water for injections 900 ml, sodium chloride 7.5 g, water for injections ad 1000 ml; the pH was adjusted with HCl / NaOH.

Finafloxacin HCl was gradually added to 100 ml of the aqueous solutions and the pH was then readjusted until the added finafloxacin HCl did not dissolve. pH 7.5 pH 8.0 pH 8.5 pH 9.0 0.01 M Tris 6.0 mg / ml 15.0 mg / ml > 28 mg / ml > 28 mg / ml 0.025 M phosphate 2.0 mg / ml 4.0 mg / ml 6.0 mg / ml 8.0 mg / ml WfI, pH adjusted 2.0 mg / ml 4.0 mg / ml 6.0 mg / ml 6.0 mg / ml

The results of Example 1 clearly demonstrate the significantly improved solubility of finafloxacin in Tris. While the solubility in WFI and phosphate buffer was comparatively low, the use of 0.01M Tris resulted in a 3 to 4-fold increase in solubility. The results further show that the solubility of finafloxacin is pH dependent.

Example 2: Solubility of finafloxacin HCl in various concentrations of Tris solutions

0.25 M Tris: water for injections 800 ml, 30.3 g Tris, sodium chloride 7.5 g, water for injections ad 1000 ml; the pH was adjusted with HCl / NaOH.

0.17 M Tris: water for injections 800 ml, 20.0 g Tris, sodium chloride 7.5 g, water for injections ad 1000 ml; the pH was adjusted with HCl / NaOH.

0.08 M Tris: water for injections 800 ml, 10.0 g Tris, sodium chloride 7.5 g. Water for injections ad 1000 ml; the pH was adjusted with HCl / NaOH.

Finafloxacin HCl was added gradually to 100 ml of the aqueous solutions until the added finafloxacin HCl did not dissolve. In contrast to Example 1, the pH was not readjusted after the stepwise addition of finafloxacin. 0.08 M Tris 0.17 M Tris 0.25 M Tris pH 7.0 0 mg / ml 0 mg / ml 0 mg / ml pH 7.4 0 mg / ml 2.0 mg / ml 2.0 mg / ml pH 7.8 4.0 mg / ml 6.0 mg / ml 8.0 mg / ml pH 8.2 6.0 mg / ml 10.0 mg / ml 15.0 mg / ml pH 8.6 9.0 mg / ml 19.0 mg / ml 24.0 mg / ml pH 9.0 10.0 mg / ml 23.0 mg / ml 28.0 mg / ml

The results show that the solubility of finafloxacin is dependent on the Tris concentration. The above results generally show a lower solubility of finafloxacin than in Example 1, since the pH was not readjusted after the stepwise addition of finafloxacin.

Example 3: Stability of finafloxacin compositions containing Tris

The following composition was used to test the stability: component Quantity (g / l) function Finafloxacin 3.2 active substance NaCl 7.8 vehicle Tris 1.21 Solubility enhancing ingredient NaOH 1 M (for pH adjustment to 8.25) qs pH adjustment HCl 1 M (for pH adjustment to 8.25) qs pH adjustment Water for injections to 1 liter solvent qs - quantum satis means the use of "as much as necessary" substance.

Solutions prepared according to this formulation showed a long-term stability of at least 24 months.

Example 4: Effectiveness of finafloxacin compositions containing Tris

• 4.1 Die Bakterien wurden in einer Finafloxacin Zusammensetzung mit 0,05 M Tris bei pH 8,0 inkubiert und die minimale Hemmkonzentration (MHK) von Finafloxacin, definiert als die minimale Finafloxacin-Konzentration, die das Wachstum des Bakteriums inhibiert, wurde bestimmt unter Verwendung einer gängigen in vitro Empfindlichkeitsprüfung. Die MHK für S. aureus 29213 betrug 0,5 µg/ml und die MHK für E. coli 25922 betrug 0,25 µg/ml.
• 4.2 Mäuse wurden mit jeweils 3,9 × 10⁵ E. coli ATCC 25922, suspendiert in 1% Schweine-Mucin, durch eine 0,5 ml intraperitoneale Injektion infiziert. Die antibakterielle Behandlung mit einer Finafloxacin-Zusammensetzung, die 0,01 M Tris beinhaltete, wurde 4 Stunden nach der Infektion initiiert. Eine zweite Dosis wurde 12 Stunden nach der Infektion verabreicht. Die bakterielle Belastung in der Bauchflüssigkeit und in einer Blutkultur wurde 24 Stunden nach der Infektion bestimmt. Finafloxacin war bei allen getesteten Dosen wirksam. Dabei wurde bei 1 mg/kg eine Verringerung der Bakterienlast von 3,1 log10 koloniebildenden Einheiten/g erreicht. Finafloxacin, welches mit Dosen von 3, 10 und 30 mg/kg verabreicht wurde, zeigte eine konstant ansteigende Effektivität durch weitere Absenkungen der Bakterienlast auf 4,4; 5,0 und 6,5 log10 KBE/g.
• 4.3 Patienten mit komplizierten Harnweginfektionen und Pyelonephritis wurden mit einer intravenösen Dosis von 800 mg Finafloxacin einmal täglich behandelt. 17 Tage nach dem Start der Therapie wurden die mikrobiologischen Behandlungsergebnisse bestimmt. Mikrobiologische Heilung wurde definiert als die Reduzierung der Konzentration des Pathogen im Urin auf einen Titer von ≤ 10³ koloniebildenden Einheiten/ml. Die Finafloxacin Zusammensetzung, die 0,01 M Tris umfasste, führte zu einer nachhaltigen Abtötung der Pathogene. Die mikrobiologischen Heilungsrate betrug 83%.

The efficacy of finafloxacin compositions containing Tris was examined between pH 8.0 to 8.5 and determined as follows:

• 4.1 The bacteria were incubated in a finafloxacin composition with 0.05 M Tris at pH 8.0 and the minimum inhibitory concentration (MIC) of finafloxacin, defined as the minimum finafloxacin concentration that inhibits the growth of the bacterium, was determined using a common in vitro susceptibility testing. The MIC for S. aureus 29213 was 0.5 μg / ml and the MIC for E. coli 25922 was 0.25 μg / ml.
• 4.2 mice were infected with 3.9 x 10 ⁵ E. coli ATCC 25922, suspended in 1% porcine mucin, by a 0.5 ml intraperitoneal injection. Antibacterial treatment with a finafloxacin composition containing 0.01 M Tris was initiated 4 hours after infection. A second dose was given 12 hours after infection. The bacterial load in the abdominal fluid and in a blood culture was determined 24 hours after the infection. Finafloxacin was effective at all doses tested. At 1 mg / kg, a reduction in bacterial load of 3.1 log10 colony-forming units / g was achieved. Finafloxacin, administered at doses of 3, 10 and 30 mg / kg, showed a constant increase in effectiveness by further reducing the bacterial load to 4.4; 5.0 and 6.5 log10 cfu / g.
• 4.3 Patients with complicated urinary tract infections and pyelonephritis were treated with an intravenous dose of 800 mg finafloxacin once daily. 17 days after the start of the therapy, the microbiological treatment results were determined. Microbiological healing has been defined as the reduction of the concentration of urinary pathogen to a titer of ≤10 ³ colony forming units / ml. The finafloxacin composition, which included 0.01 M Tris, resulted in a sustained killing of the pathogens. The microbiological cure rate was 83%.

Example 5: Safety of Finafloxacin Compositions Having Tris

Doses of 60, 120 and 200 mg finafloxacin / kg / day were given intravenously to rats for 2 weeks. According to the toxicological assessment of the animals during the course of the study, these doses were generally well tolerated. Finafloxacin was formulated in 0.01 M Tris, 0.75% (w / v) sodium chloride and adjusted to pH 8.5 in water for injection.

QUOTES INCLUDE IN THE DESCRIPTION

This list of the documents listed by the applicant has been generated automatically and is included solely for the better information of the reader. The list is not part of the German patent or utility model application. The DPMA assumes no liability for any errors or omissions.

Cited patent literature

• WO 98/26779 [0002, 0003]
• EP 0946176 [0002, 0003]
• US 8536167 [0002, 0003]

Claims (22)

 Composition comprising finafloxacin and tris. A composition according to claim 1, wherein the composition comprises Tris in a concentration of 0.001 M to 0.2 M, preferably in a concentration of 0.002 M to 0.1 M, particularly preferably in a concentration of 0.01 M. A composition according to claim 1 or 2, wherein the composition has a pH of 7.0 to 12.0, preferably a pH of 8.0 to 10.0, more preferably a pH of 8.0 to 8.5, having. A composition according to any one of claims 1 to 3, wherein the composition is a pharmaceutically acceptable composition for parenteral use. A composition according to any one of claims 1 to 4, wherein the composition additionally comprises a pharmaceutical excipient. Composition according to claim 5, wherein the composition is particularly preferred sodium chloride in a concentration of 0.4% to 1.0% (w / v), preferably in a concentration of 0.6% to 0.9% (w / v) in a concentration of 0.7% to 0.8% (w / v). A composition according to any one of claims 1 to 6, wherein the composition has an osmolality of 200 to 700 mOsmol / kg, preferably an osmolality of 260 to 390 mOsmol / kg, more preferably an osmolality of 270 to 350 mOsmol / kg. A composition according to any one of claims 1 to 7, wherein the composition contains finafloxacin monohydrochloride. A composition according to any one of claims 1 to 8, wherein the composition is finafloxacin at a concentration of from 0.2 g / l to 50 g / l, preferably at a concentration of from 0.4 g / l to 25 g / l, more preferably in one Concentration of 0.8 g / l to 13 g / l. A composition according to any one of claims 1 to 9, wherein the composition comprises 1.6 to 6.4 g / L finafloxacin, 7 to 8 g / L NaCl, 1 to 2 g / L Tris and a pH of 8.0 to 8, 5 has. The composition of claim 10, wherein the composition comprises 3.2 g / L finafloxacin, 7.8 g / L NaCl, 1.21 g / L Tris and has a pH of 8.25. A composition according to any one of claims 4 to 11 for use in the treatment of bacterial infections. A composition for use according to claim 12 for use in the treatment of urinary tract infections and pyelonephritis. A composition for use according to claim 12 for use in the treatment of intra-abdominal infections.  A composition for use according to claim 12 for use in the treatment of skin and soft tissue infections. A composition for use according to claim 12 for use in the treatment of the diabetic foot. A composition for use according to claim 12 for use in the treatment of bacteremia. A composition for use according to claim 12 for use in the treatment of respiratory tract infection. A composition for use according to claim 12 for use in the treatment of prostatitis. A composition for use according to claim 12 for use in the treatment of bone and joint infections. A composition according to any one of claims 4 to 11 for use in a method of preventing bacterial infections in mammals and humans. Use of a pharmaceutically effective amount of a composition according to any one of claims 4 to 11 in the manufacture of a medicament for the treatment of bacterial infections.